The N-myc and C-myc Downstream Pathways Include the Chromosome 17q Genes Nm23-H1 and Nm23-H2

Overview

Journal Oncogene

Specialties Molecular Biology
Oncology

Date 2002 Apr 18

PMID 11960382

Citations 24

Authors

Marc B Godfried

Monique Veenstra

Peter V Sluis

Kathy Boon

Ronald v Asperen

Marie Christien Hermus

Barbara D C v Schaik

Tom P A Voute

Manfred Schwab

Rogier Versteeg

Huib N Caron

Affiliations

Soon will be listed here.

Abstract

Gain of chromosome 17q material is the most frequent genetic abnormality in neuroblastomas. The common region of gain is at least 375 cR large, which has precluded the identification of genes with a role in neuroblastoma pathogenesis. Neuroblastoma also frequently show amplification of the N-myc oncogene, which correlates closely with 17q gain. Both events are strong predictors of unfavorable prognosis. To identify genes that are part of the N-myc downstream pathway, we constructed SAGE libraries of an N-myc transfected and a control cell line. This identified the chromosome 17q genes nm23-H1 and nm23-H2 as being 6-10 times induced in the N-myc expressing cells. Northern and Western blot analysis confirmed this up-regulation. Time-course experiment shows that both genes are induced within 4 h after N-myc is switched on. Furthermore, we demonstrate also that c-myc can up-regulate nm23-H1 and nm23-H2 expression. Neuroblastoma tumor and cell line panels reveal a striking correlation between N-myc amplification and mRNA and protein expression of both nm23 genes. We show that the nm23 genes are located at the edge of the common region of chromosome 17q gain previously described in neuroblastoma cell lines. Our findings suggest that nm23-H1 and nm23-H2 expression is increased by 17q gain in neuroblastoma and can be further up-regulated by myc overexpression. These observations suggest a major role for nm23-H1 and nm23-H2 in tumorigenesis of unfavorable neuroblastomas.

Citing Articles

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